Signalling by Src family kinases: Lessons learnt from DNA tumour viruses

被引：11

作者：

Dunant, N ^{[1
]}

BallmerHofer, K ^{[1
]}

机构：

[1] FRIEDRICH MIESCHER INST, CH-4002 BASEL, SWITZERLAND

来源：

CELLULAR SIGNALLING | 1997年 / 9卷 / 06期

关键词：

Src family kinases; polyomavirus; Epstein-Barr virus; herpesvirus Saimiri; Middle-T; Lmp2; Tip;

D O I：

10.1016/S0898-6568(97)00040-5

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

Virus replication and spreading in a host population depends on highly specific interactions of viral proteins with infected cells, resulting in subversion of multiple cellular signal transduction pathways. For instance, viral proteins cause cell cycle progression of the infected host cell in order to establish a cellular environment favourable for virus replication. Of equal importance for successful virus propagation is virus mediated attenuation of a host's immune response. Many of the pathways controlling these aspects of cell behaviour are regulated by cellular tyrosine kinases. One particular family of these enzymes, Src family kinases, are involved in processing signals emanating from the plasma membrane upon stimulation by growth factors, by cell substratum or by cell-cell contact. Two families of DNA viruses, polyoma-and herpesviruses, encode proteins targeted at tyrosine kinases. The middle-T antigens expressed by mouse and hamster polyomavirus associate with and activate Src family tyrosine kinases. Two members of the herpes family of DNA viruses, Epslein-Barr virus (EBV) and herpesvirus saimiri (HVS), encode proteins, LMP2A and Tip, respectively, that associate with cellular tyrosine kinases of the Src and Syk/Zap family. Upon association with these viral proteins, the activity of these tyrosine kinases is changed resulting in altered signal output. Middle-T, LMP2A and Tip are therefore excellent tools to study the regulation of Src family kinases. (C) 1997 Elsevier Science Inc.

引用

页码：385 / 393

页数：9

共 126 条

[1] SH3 DOMAINS SPECIFICALLY REGULATE KINASE-ACTIVITY OF EXPRESSED SRC FAMILY PROTEINS
ABRAMS, CS
ZHAO, W
[J]. JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (01) : 333 - 339
[2] PROLINE-RICH SEQUENCES THAT BIND TO SRC HOMOLOGY-3 DOMAINS WITH INDIVIDUAL SPECIFICITIES
ALEXANDROPOULOS, K
CHENG, GH
BALTIMORE, D
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (08) : 3110 - 3114
[3] AVILA LT, 1981, VIROLOGY, V114, P501
[4] ALTERED TYROSINE-527 PHOSPHORYLATION AND MITOTIC ACTIVATION OF P60C-SRC
BAGRODIA, S
CHACKALAPARAMPIL, I
KMIECIK, TE
SHALLOWAY, D
[J]. NATURE, 1991, 349 (6305) : 172 - 175
[5] MYC BUT NOT FOS RESCUE OF PDGF SIGNALING BLOCK CAUSED BY KINASE INACTIVE SRC
BARONE, MV
COURTNEIDGE, S
[J]. NATURE, 1995, 378 (6556) : 509 - 512
[6] BASTIEN C, 1988, ONCOGENE, V2, P129
[7] THE (YXXL/I)(2) SIGNALING MOTIF FOUND IN THE CYTOPLASMIC SEGMENTS OF THE BOVINE LEUKEMIA-VIRUS ENVELOPE PROTEIN AND EPSTEIN-BARR-VIRUS LATENT MEMBRANE PROTEIN-2A CAN ELICIT EARLY AND LATE LYMPHOCYTE-ACTIVATION EVENTS
BEAUFILS, P
CHOQUET, D
MAMOUN, RZ
MALISSEN, B
[J]. EMBO JOURNAL, 1993, 12 (13) : 5105 - 5112
[8] THE PRODUCT OF THE HERPESVIRUS-SAIMIRI OPEN READING FRAME-1 (TIP) INTERACTS WITH T-CELL-SPECIFIC KINASE P56(LCK) IN TRANSFORMED-CELLS
BIESINGER, B
TSYGANKOV, AY
FICKENSCHER, H
EMMRICH, F
FLECKENSTEIN, B
BOLEN, JB
BROKER, BM
[J]. JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (09) : 4729 - 4734
[9] STABLE GROWTH TRANSFORMATION OF HUMAN LYMPHOCYTES-T BY HERPESVIRUS SAIMIRI
BIESINGER, B
MULLERFLECKENSTEIN, I
SIMMER, B
LANG, G
WITTMANN, S
PLATZER, E
DESROSIERS, RC
FLECKENSTEIN, B
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1992, 89 (07) : 3116 - 3119
[10] ENHANCEMENT OF CELLULAR SRC GENE-PRODUCT ASSOCIATED TYROSYL KINASE-ACTIVITY FOLLOWING POLYOMA-VIRUS INFECTION AND TRANSFORMATION
BOLEN, JB
THIELE, CJ
ISRAEL, MA
YONEMOTO, W
LIPSICH, LA
BRUGGE, JS
[J]. CELL, 1984, 38 (03) : 767 - 777

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